| Literature DB >> 30664780 |
Vitor H Teixeira1, Christodoulos P Pipinikas1,2, Adam Pennycuick1, Henry Lee-Six3, Deepak Chandrasekharan1, Jennifer Beane4, Tiffany J Morris2, Anna Karpathakis2, Andrew Feber2, Charles E Breeze2, Paschalis Ntolios1, Robert E Hynds1,5,6, Mary Falzon7, Arrigo Capitanio7, Bernadette Carroll8, Pascal F Durrenberger9, Georgia Hardavella8, James M Brown1, Andy G Lynch10,11, Henry Farmery10, Dirk S Paul2, Rachel C Chambers9, Nicholas McGranahan5, Neal Navani1,8, Ricky M Thakrar1,8, Charles Swanton5,6, Stephan Beck2, Phillip Jeremy George8, Avrum Spira4,12, Peter J Campbell3, Christina Thirlwell2, Sam M Janes13,14.
Abstract
The molecular alterations that occur in cells before cancer is manifest are largely uncharted. Lung carcinoma in situ (CIS) lesions are the pre-invasive precursor to squamous cell carcinoma. Although microscopically identical, their future is in equipoise, with half progressing to invasive cancer and half regressing or remaining static. The cellular basis of this clinical observation is unknown. Here, we profile the genomic, transcriptomic, and epigenomic landscape of CIS in a unique patient cohort with longitudinally monitored pre-invasive disease. Predictive modeling identifies which lesions will progress with remarkable accuracy. We identify progression-specific methylation changes on a background of widespread heterogeneity, alongside a strong chromosomal instability signature. We observed mutations and copy number changes characteristic of cancer and chart their emergence, offering a window into early carcinogenesis. We anticipate that this new understanding of cancer precursor biology will improve early detection, reduce overtreatment, and foster preventative therapies targeting early clonal events in lung cancer.Entities:
Mesh:
Year: 2019 PMID: 30664780 DOI: 10.1038/s41591-018-0323-0
Source DB: PubMed Journal: Nat Med ISSN: 1078-8956 Impact factor: 53.440